[ ]	REGISTRATION STATEMENT PURSUANT TO SECTION 12(b) OR (g) OF THE SECURITIES EXCHANGE ACT OF 1934; or
[ X ]	ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934
	For the fiscal year ended November 30, 2010; or
[ ]	TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934; or
[ ]	SHELL COMPANY REPORT PURSUANT TO SECTION 13 OR 15(d) OF THE SECURITIES EXCHANGE ACT OF 1934 Date of event requiring this shell company report …………
	For the transition period from ________ to ________

 

 

 

 

 

 

 

Title of each class		Name of each exchange on which registered
Common shares, no par value		NASDAQ TSX

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

U.S. GAAP [x]

International Financial Reporting Standards as issued by the International Accounting Standards Board [ ]

Other [ ]

 

 

 

 

 

 

 

 

 

 

 

A.	Directors and senior management

 

 

B.

Advisors

 

 

C.

Auditors

 

Not applicable.

 

 

 

 

A.	Selected Financial Data

 

 

Periods ended (in thousands of US dollars, except for per share data)
	As at and for the year ended November 30, 2010		As at and for the eleven month period ended November 30, 2009	As at and for the year ended December 31, 2008		As at and for the year ended December 31, 2007		As at and for the year ended December 31, 2006
Revenue	1,459		630	1,278		2,297		1,490
Loss for the period	(5,761)		(1,839)	(3,765)		(1,291)		(1,320)
Total assets	3,268		11,081	3,026		6,878		3,027
Total liabilities	3,175		6,449	3,609		4,557		2,567
Net assets	93		4,632	(583)		2,322		460
Capital stock	17		17	17		17		17
Loss per share - basic and diluted	(0.53)		(0.19)	(0.40)		(0.14)		(0.15)
Dividends	Nil		Nil	Nil		Nil		Nil
Weighted average common shares	10,907		9,512	9,328		9,087		8,877

 

 

B.	Capitalization and Indebtedness

 

 

C.	Reasons for the Offer and Use of Proceeds

 

 

D.	Risk Factors

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

·

for ANDA candidates, bioequivalence studies results may not meet regulatory requirements for the demonstration of bioequivalence;

 

·

for new drug application (“NDA”) candidates, a product may not demonstrate acceptable clinical trial results, even though it demonstrated positive preclinical trial results;

 

·

for NDA candidates, a product may not be effective in treating a specified condition or illness;

 

·

a product may have harmful side effects on humans;

 

·

products may fail to receive the necessary regulatory approvals from the FDA or other regulatory bodies, or there may be delays in receiving such approvals.  Among other things, such delays may be caused by slow enrolment in clinical studies, extended lengths of time to achieve study endpoints, additional time requirements for data analysis, discussions with the FDA, FDA requests for additional preclinical or clinical data, or unexpected safety, efficacy or manufacturing issues;

 

·

difficulties may be encountered in formulating products, scaling up manufacturing processes or in getting approval for manufacturing;

 

·

manufacturing costs, pricing or reimbursement issues, other competitive therapeutics, or other commercial factors may make the product uneconomical; and

 

·

the proprietary rights of others, and their competing products and technologies, may prevent the product from being developed or commercialized.

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

·

the availability of alternative products from competitors;

 

·

the prices of our products relative to those of our competitors;

 

·

the timing of our market entry;

 

·

the ability to market our products effectively at the retail level; and

 

·

the acceptance of our products by government and private formularies.

 

 

 

 

 

 

 

 

 

·

delays in patient enrolment, and variability in the number and types of patients available for  clinical trials;

 

·

regulators or institutional review boards may not allow us to commence or continue a clinical trial;

 

·

our inability, or the inability of our partners, to manufacture or obtain from third parties materials sufficient to complete our clinical trials;

 

·

delays or failures in reaching agreement on acceptable clinical trial contracts or clinical trial protocols with prospective clinical trial sites;

 

·

risks associated with trial design, which may result in a failure of the trial to show statistically significant results even if the product candidate is effective;

 

·

difficulty in maintaining contact with patients after treatment commences, resulting in incomplete data;

 

·

poor effectiveness of product candidates during clinical trials;

 

·

safety issues, including adverse events associated with product candidates;

 

·

the failure of patients to complete clinical trials due to adverse side effects, dissatisfaction with the product candidate, or other reasons;

 

·

governmental or regulatory delays or changes in regulatory requirements, policy and guidelines; and

 

·

varying interpretation of data by the FDA or other applicable foreign regulatory agencies.

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

·

Contract manufacturers can encounter difficulties in achieving volume production, quality control and quality assurance, or technology transfer, as well as shortages of qualified personnel. Accordingly, a manufacturer might not be able to manufacture sufficient quantities to meet our clinical trial needs or to commercialize our products.

 

·

Contract manufacturers are required to undergo a satisfactory cGMP inspection prior to regulatory approval and are obliged to operate in accordance with the cGMP regulations of the FDA regulations and those of other jurisdictions we may manufacture in or apply for approval for some of our products.  These regulations govern manufacturing processes, stability testing, record keeping and quality standards. Any failure of these contract manufacturers to establish and follow cGMP or other similar applicable regulations and to document their adherence to such practices may lead to significant delays in the availability of material for clinical studies, may delay or prevent filing or approval of marketing applications for our products or result in sanctions being imposed on us.

 

·

For some or all of our current product candidates and possibly for any future products, we may initially rely on a single or a limited number of contract manufacturers. Changing these or future manufacturers may be difficult and the number of potential manufacturers is limited. Changing manufacturers generally requires re-validation of the manufacturing processes and procedures in accordance with FDA and other applicable national cGMPs and may require prior regulatory approval. It may be difficult or impossible for us to quickly find replacement manufacturers on acceptable terms, if at all. Such re-validation may be costly and time-consuming and we could suffer important delays in advancing our product candidates in clinical trials or in supplying the commercial market with our products.

 

·

With respect to any of our products that we may market, our ability to reach full commercial scale manufacturing depends upon the ability of our own plant or a designated commercial scale contract manufacturer to be approved under such cGMP. Reaching full commercial scale has a direct impact on our overall costs of goods, which, in turn, directly affects our operating margins. Any delay in obtaining cGMP approval beyond the time we anticipate may have a negative impact on our operating margins and other financial results, as well as our ability to adequately supply the market with our product.

 

·

Our contract manufacturers may not perform as agreed or may not remain in the contract manufacturing business for the time required to produce, store and distribute our products successfully.

 

·

Our contract manufacturers may terminate or not renew our agreements based on their own priorities and such actions could be both costly and inconvenient for us.

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

·

varying regulatory restrictions on sales of our products to certain markets and unexpected changes in regulatory requirements;

 

·

tariffs, customs, duties, and other trade barriers;

 

·

difficulties in managing foreign operations and foreign distribution partners;

 

·

longer payment cycles and problems in collecting accounts receivable;

 

·

fluctuations in currency exchange rates;

 

·

political risks;

 

·

foreign exchange controls that may restrict or prohibit repatriation of funds;

 

·

export and import restrictions or prohibitions, and delays from customs brokers or government agencies;

 

·

seasonal reductions in business activity in certain parts of the world; and

 

·

potentially adverse tax consequences.

 

 

 

 

 

 

 

·

sales or other issuances of our common shares, including any sales made in connection with future financings;

 

·

announcements regarding new or existing corporate partnerships;

 

·

announcements by us of significant acquisitions, joint ventures, or capital commitments;

 

·

actual or anticipated period-to-period fluctuations in financial results;

 

·

clinical and regulatory development regarding our product candidates;

 

·

litigation or threat of litigation;

 

·

failure to achieve, or changes in, financial estimates by securities analysts;

 

·

comments or opinions by securities analysts or members of the medical community;

 

·

announcements regarding new or existing products or services or technological innovations by us or our competitors;

 

·

conditions or trends in the pharmaceutical and biotechnology industries;

 

·

additions or departures of key personnel or directors;

 

·

economic and other external factors or disasters or crises;

 

·

limited daily trading volume; and

 

·

developments regarding our patents or other intellectual property or that of our competitors.

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

·

must make a special written suitability determination for the purchaser;

 

·

receive the purchaser’s written agreement to a transaction prior to sale;

 

·

provide the purchaser with risk disclosure documents which identify risks associated with investing in “penny stocks” and which describe the market for these “penny stocks” as well as a purchaser’s legal remedies; and

 

·

obtain a signed and dated acknowledgment from the purchaser demonstrating that the purchaser has actually received the required risk disclosure document before a transaction in a “penny stock” can be completed.

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

A.	History and Development of the Company

 

 

 

 

 

 

 

 

 

B.	Business Overview

 

 

 

 

 

·

For existing controlled-release (once-a-day) products covered by patents about to expire or already expired, we can formulate generic products, which are bioequivalent to the branded products. Such products can be licensed to and sold by distributors of generic products.  Our scientists have previously developed several drugs which have been commercialized in the United States by their former employer/client.  The regulatory pathway for this approach requires an abbreviated new drug application (“ANDA”).

 

·

For branded immediate-release (multiple-times-per-day) drugs, we can formulate improved replacement products, typically by developing new, patentable, controlled-release once-a-day drugs. These drugs can be licensed to and sold by the pharmaceutical company that made the original immediate-release product.  This protects against revenue erosion in the brand by providing a clinically attractive patented product that competes favorably with the generic immediate-release competition that arises on expiry of the original patent(s). The regulatory pathway for this approach requires new drug applications (“NDA”) via 505(b)(2) application which both accelerates development timelines and reduces costs in comparison to regular new drug applications for new chemical entities.

 

·

Our technologies are also focused on the development of abuse-deterrent pain medications. The growing abuse and diversion of prescription “painkillers”, specifically opioid analgesics, is well documented and is a major health and social concern. We believe that our technologies and know-how are uniquely suited to developing abuse-deterrent pain medications.

 

 

 

 

 

 

 

 

 

 

·

For existing controlled-release (once-a-day) products covered by patents about to expire or already expired, we can seek to formulate generic products which are bioequivalent to the branded products. Our scientists have done so previously for several drug products, on a private contract basis with third-party companies that cannot be disclosed because of confidentiality obligations of our scientists under their prior development agreements. Such products may be licensed to and sold by distributors of generic products.

 

·

For branded immediate-release (multiple-times-per-day) products, we can seek to formulate improved replacement products, typically by developing a new, patentable, controlled-release (once-a-day) product.  Such products may be licensed to and sold by the pharmaceutical company that made the original immediate-release product, thereby protecting the pharmaceutical company against revenue loss in the brand by providing a clinically attractive patented product that is expected to compete favourably with the generic immediate-release competition that arises on expiry of the original patent(s).

 

·

Our technologies are also focused on the development of abuse-deterrent pain medications. The growing abuse and diversion of prescription “painkillers”, specifically opioid analgesics, is well documented and is a major health and social concern. We believe that our technologies and know-how are uniquely suited to developing abuse-deterrent pain medications.

 

 

·

Our delivery technologies offer competitive development times.  They have demonstrated themselves suited to the delivery of a wide range of small molecule drugs.  They are robust in that the predicted delivery results have been repeatedly substantiated by actual bioavailability/bioequivalence studies.  They were developed by our chief scientists, who have substantial experience in applying them successfully to the delivery of small drug molecules under existing development contracts and in support of our pipeline.  For these reasons, we believe that our development times are relatively short and competitive.

 

·

Our delivery technologies offer competitive development costs, because the technologies use only readily available, low-cost ingredients already acceptable to regulatory authorities such as the FDA, and because development times are short, we believe in the opinion of management our development costs are low when compared to our competitors.

 

·

Large pharmaceutical companies may license our improved products for life-cycle management and franchise extension of their branded products as they come off patent.  Our management believes that, with impending loss of branded product revenues, a new generic version of that product such as we develop, which offers the advantage of once-a-day dosing, should be attractive to a large pharmaceutical company facing revenue loss in a patented branded-product franchise.

 

·

Manufacturers and distributors of generic drugs may license our technologies and products.  Because our development times are, in our opinion comparatively short and cost-effective, our generic once-a-day products represent a cost-effective opportunity for generic distributors to add valuable generic products to their portfolios.

 

 

 

1.

In May 2007, we filed an ANDA with the FDA for 5mg, 10mg, 15mg and 20mg strengths of generic Focalin XR® developed in collaboration with partner, Par Pharmaceutical and intended for the U.S. market. In August 2007, the application was accepted by the FDA as being complete and in condition for further review. In December 2010, we filed an ANDA for the 30mg strength of generic Focalin XR®, which is not partnered.

 

2.

In May 2010, our ANDA filing for generic Effexor XR® was accepted by the FDA for review.

 

3.

In June 2010, our ANDA filing for generic Protonix® was accepted by the FDA for review.

 

4.

In October 2010, our ANDA filing for generic Glucophage® XR was accepted by the FDA for review.

 

5.

In February 2011, our ANDA filing for generic Seroquel XR® was accepted by the FDA for review.

 

·

The ANDA review process generally takes at least two years and often longer, and there can be no assurance that the FDA will approve the product for commercial launch in the USA.

 

·

Commercial exploitation of these products either by license and the collection of royalties, or through the manufacture of tablets and capsules using our developed formulations.

 

·

Development of new products and increasing the number of licensing agreements with other pharmaceutical companies beyond those already in place, including collaborating in contract research and development, joint ventures and other drug development and commercialization projects.

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

Generic name	Brand	Indication	Stage of Development	Regulatory Pathway	Rights
Dexmethylphenidate hydrochloride extended-release capsules	Focalin XR®	Attention-deficit hyperactivity disorder	Application under review by the FDA for 5mg, 10mg, 15mg, 20mg strength ANDA for 30mg dosage strength filed as an amendment	ANDA	Intellipharmaceutics and Par Pharmaceutical
Venlafaxine hydrochloride extended-release capsules	Effexor XR®	Depression	Application under review by the FDA	ANDA	Intellipharmaceutics
Pantoprazole sodium delayed-release capsules	Protonix®	Conditions associated with gastroesophageal reflux disease	Application under review by the FDA	ANDA	Intellipharmaceutics
Metformin hydrochloride extended-release capsules	Glucophage®XR	Management of type 2 diabetes	Application under review by the FDA	ANDA	Intellipharmaceutics
Quetiapine fumarate extended-release tablets	Seroquel XR®	Schizophrenia, bipolar disorder, and major depressive disorder	Application under review by the FDA	ANDA	Intellipharmaceutics
Carvedilol phosphate extended-release capsules	Coreg CR®	Heart failure, hypertension	Late-stage development	ANDA	Intellipharmaceutics
Oxycodone hydrochloride controlled-release capsules	N/A	Pain	Early-stage development	NDA 505(b)(2)	Intellipharmaceutics

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

Country	Issue No.	Issue Date	Title
U.S.A.	6,652,882	November 25, 2003	Controlled Release Formulation Containing Bupropion
U.S.A.	6,296,876	October 2, 2001	Pharmaceutical Formulations for Acid Labile Substances
U.S.A.	6,607,751	August 19, 2003	Novel Controlled Release Delivery Device for Pharmaceutical Agents Incorporating Microbial Polysaccharide Gum
U.S.A.	6,479,075	November 12, 2002	Pharmaceutical Formulations for Acid Labile Substances

 

 

 

 

 

 

 

 

In certain cases, where the objective is to develop a generic version of an approved product already on the market in controlled-release dosages, an ANDA may be filed in lieu of filing an NDA.  Under the ANDA procedure, the FDA waives the requirement to submit complete reports of preclinical and clinical studies of safety and efficacy and instead requires the submission of bioequivalency data demonstrating that the generic drug produces the same effect in the body as its brand-name counterpart and has the same pharmacokinetic profile, or change in blood concentration over time.  The ANDA procedure is available to us for a generic version of a drug product approved by the FDA.  In certain cases, an ANDA applicant may submit a suitability petition to the FDA requesting permission to submit an ANDA for a drug product that differs from a previously approved reference drug product (the “Listed Drug”) when the change is one authorized by statute.  Permitted variations from the Listed Drug include changes in: (1) route of administration, (2) dosage form, (3) strength and (4) one of the active ingredients of the Listed Drug when the Listed Drug is a combination product.  The FDA must approve the petition before the ANDA may be submitted.  An applicant is not permitted to petition for any other kinds of changes from Listed Drugs.  The information in a suitability petition must demonstrate that the change from the Listed Drug requested for the proposed drug product may be adequately evaluated for approval without data from investigations to show the proposed drug product’s safety or effectiveness.  The advantages of an ANDA over an NDA include reduced research and development costs associated with bringing a product to market, and generally a shorter review and approval time at the FDA.

 

 

 

 

 

 

 

 

 

 

 

The Canadian government has regulations which can prohibit the issuance of an NOC for a patented medicine to a generic competitor, provided that the patentee or an exclusive licensee has filed a list of its Canadian patents covering that medicine with the Minister of Health and Welfare.  After submitting the list, the patentee or an exclusive licensee can commence a proceeding to obtain an order of prohibition directed to the Minister prohibiting him or her from issuing an NOC.  The minister may be prohibited from issuing an NOC permitting the importation or sale of a patented medicine to a generic competitor until patents on the medicine expire or the waiver of infringement and/or validity of the patent(s) in question is resolved by litigation in the manner set out in such regulations.  There may be additional patents relating to a company’s proposed manufacture, use or sale of a product that could potentially prohibit such company’s proposed commercialization of a drug compound.

 

 

C.	Organizational Structure

 

 

 

 

 

A.	Operating Results

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

Gain on foreign exchange was $138,949 for the year ended November 30, 2010 in comparison to a gain of $587,642 for the eleven month period ended November 30, 2009. The decrease for the year ended November 30, 2010 was due to the decrease of the US dollar against the Canadian dollar as the rates changed from $1.00 (US) for $1.0266 (Cdn) at November 30, 2010, from $1.00 (US) for $1.0556 (Cdn) at November 30, 2009, and from $1.00(US) for $1.2180 (Cdn) at December 31, 2008. During the year ended November 30, 2010 the exchange rate averaged $1.00 (US) for $1.0345 (Cdn) compared to $1.00 (US) for $1.1493 (Cdn) for the eleven months ended November 30, 2009.

 

 

 

 

 

 

 

 

 

 

Expenditure for wages and benefits for the eleven month period ended November 30, 2009 were $338,110 compared with $373,717 for the year ended December 31, 2008. This reduction is attributable to a decrease in administrative staffing levels and salary reductions during the eleven month period ending November 30, 2009 when compared to the prior period.

 

 

 

 

 

 

 

 

 

 

B.	Liquidity and Capital Resources

 

The Company had cash of $789,136 as at November 30, 2010 compared to $8,014,492 as at November 30, 2009, and compared to $902,213 at December 31, 2008. The decrease in cash during the year ended November 30, 2010 is mainly a result of cash used in operating activities and the repayment of C$910,000 of a related party loan payable to Dr. Isa Odidi and Dr. Amina Odidi. The increase in cash during the period ended November 30, 2009 is a result of the transactions, as described in the “Business Overview”, effective October 22, 2009 which resulted in us receiving $11.0 million in cash and an additional $0.5million in receivables from tax credits recoverable that were earned by Vasogen from the Ontario Innovation Tax Credit, the Goods and Services Tax Credits and other recoverable tax amounts.

 

 

 

 

 

 

 

The Company received C$640,081 from the Canada Revenue Agency and the Ontario Ministry of Finance during the first quarter of fiscal 2011 comprised of research and development investment tax credits for research and development activities carried out to the period ended October 21, 2009. During the first half of fiscal 2011, the Company expects to receive a substantial portion of approximately C$380,000 in other tax credits receivable that were acquired in the October 22, 2009 IPC Arrangement Transaction. In addition, based on management’s estimate, the Company expects to file a refundable claim of approximately C$226,000 for the investment tax credit with the Ontario Ministry of Finance in the second quarter of fiscal 2011 for research and development activities carried out during the fiscal year 2010. Realization of these credits is subject to government approval.

 

 

C.	Research and development, patents, and licenses, etc.

 

 

 

D.	Trend Information

 

 

 

Quarter Ended		Revenues $	Loss $	Loss per share ($)
November 30, 2010		7,164	(1,903,629)	(0.18)
August 31, 2010		-	(2,113,462)	(0.19)
May 31, 2010		1,449,624	(316,447)	(0.03)
February 28, 2010		2,597	(1,427,553)	(0.13)
November 30, 2009	(2 Months)	161,757	(875,322)	(0.09)
September 30, 2009		125,590	(165,739)	(0.02)
June 30, 2009		118,460	(224,662)	(0.02)
March 31, 2009		224,372	(573,012)	(0.06)

 

E.	Off-balance sheet arrangements

 

 

F.	Contractual obligations

 

 

		Payments Due by Period
Contractual Obligations	Total	Less than 1 Year	1-3 Years	4-5 Years	After 5 Years
Capital Lease Obligations	$   13,230	$13,230	$           ---	$          ---	$          ---
Total Contractual Obligations	13,230	13,230	---	---	---

G.	Safe Harbour

 

 

·

our plans to research, develop and commercialize products and the timing of these development programs;

 

·

whether we will receive, and the timing and costs of obtaining, regulatory approvals;

 

·

development of our product candidates, including the results of current and future clinical trials or bioequivalence studies;

 

·

the benefits of our drug delivery technologies and product candidates as compared to others;

 

·

our ability to maintain and establish intellectual property rights in our drug delivery technologies and product candidates;

 

·

our need for additional financing and our estimates regarding capital requirements and future revenues and profitability;

 

·

our estimates of the size of the potential markets for product candidates;

 

·

our selection and licensing of product candidates;

 

·

our ability to attract distributors and collaborators with acceptable development, regulatory and commercialization expertise and the benefits to be derived from such collaborative efforts;

 

·

sources of revenues and anticipated revenues, including contributions from distributors and collaborators, product sales, license agreements and other collaborative efforts for the development and commercialization of product candidates;

 

·

our ability to create an effective direct sales and marketing infrastructure for products we elect to market and sell directly;

 

·

the rate and degree of market acceptance of our products;

 

·

the timing and amount of reimbursement for our products;

 

·

the success and pricing of other competing therapies that may become available;

 

·

our ability to retain and hire qualified employees;

 

·

the manufacturing capacity of third-party manufacturers that we may use for our products; and

 

·

other risk factors discussed from time to time in our reports, public disclosure documents and other filings with the securities commissions in Canada and the United States.

 

 

 

 

 

 

(1)	Member of the Audit Committee.

 

 

 

 

 

B.	Compensation

 

 

 

 

 

 

 

 

 

 

 

 

 

 

Name and principal position	Year	Salary(1)	Share-based awards	Option-based awards(2)	Non-equity incentive plan compensation		Pension value	All other compensation	Total compensation
(a)	(b)	(c)	(d)	(e)	(f)		(g)	(h)	(i)
					Annual incentive plans (f1)	Long-term incentive plans (f2)
Dr. Isa Odidi, Chairman& Chief Executive Officer	2010 2009 2008	436,997 383,481 341,134	N/A N/A N/A	Nil Nil Nil	N/A N/A N/A	N/A N/A N/A	N/A N/A N/A	11,600 8,701 11,245	448,597 392,182 352,379
Dr. Amina Odidi, President & Chief Operating Officer (3)	2010 2009 2008	436,997 383,481 341,134	N/A N/A N/A	Nil Nil Nil	N/A N/A N/A	N/A N/A N/A	N/A N/A N/A	11,600 8,701 11,245	448,597 392,182 352,379
Shamese Rampertab VP Finance & Chief Financial Officer (4)	2010	4,614	N/A	35,374	N/A	N/A	N/A	308	40,296
Graham Neil, former VP Finance & Chief Financial Officer (5)	2010	143,990	N/A	37,522	N/A	N/A	N/A	11,512	193,024

 

Notes:

 

(1)

Salaries paid by the Company to each Named Executive Officer are paid in Canadian dollars. All amounts are expressed in U.S. dollars converted at the exchange rate of U.S.$0.9667 to C$1.00 (2009 – U.S.$0.8701; 2008 – U.S.$0.9371; 2007 – U.S.$0.9309) being the average closing exchange rate quoted by the Bank of Canada for the respective periods. Salary includes all amounts paid or payable to the Named Executive Officer. Actual amount paid to each Named Executive Officer in fiscal 2010 are as disclosed in the table. In prior years the actual amounts paid to each of the Named Executive Officers were 2009-$223,197; 2008 - $290,462; and 2007 - $288,545 with the balance being

 

(2)

The Company entered into a separate acknowledgement and agreement with Drs. Isa and Amina Odidi dated October 22, 2009 to be bound by the performance based stock option agreement dated September 10, 2004 pursuant to which Drs. Isa and Amina Odidi are entitled to purchase up to 2,763,940 of the Company’s shares upon payment of U.S.$3.62 per share, subject to satisfaction of the performance vesting conditions. The value of the option-based awards represents the closing price of the common shares on the TSX at the date of grant (C$2.62 for options granted on November 22, 2010; C$3.62 for options granted on May 26, 2010) and the following weighted average assumptions: volatility 90.4%, risk-free interest rate 3.38%, expected life 6.49 years, and no dividend yield.

 

(3)	Dr. Amina Odidi was acting Chief Financial Officer until February 12, 2010.

 

(4)	Shameze Rampertab was appointed Vice President Finance and Chief Financial Officer on November 29, 2010.

 

(5)	Graham Neil was appointed Vice President Finance and Chief Financial Officer on February 12, 2010 and resigned on November 26, 2010.

 

 

 

 

The employment agreement with Dr. Isa Odidi effective September 1, 2004 entitles Dr. Isa Odidi to receive a base salary of U.S.$200,000 per year, which is paid in Canadian dollars, to be increased annually each year during the term of the agreement by twenty percent of the prior year’s salary. In addition, he is entitled to: (a) participate in the Option Plan; (b) participate in all employee benefit plans and programs; and (c) a car allowance of up to U.S.$1,000 per month. The initial term of the employment agreement was until September 30, 2007, at which time, pursuant to the terms of the agreement, the agreement was deemed to be extended automatically for an additional three-year period on the same terms and conditions (i.e. until September 30, 2010). The agreement will continue to be extended automatically for successive additional three-year periods on the same terms unless the Company gives Dr. Odidi contrary written notice at least two years prior to the date on which the agreement would otherwise be extended. See “Termination and Change of Control Benefits” below. Dr. Odidi’s employment agreement was amended on August 1, 2007 and June 8, 2009 to provide for additional intellectual property and non-competition provisions and to provide for non-solicitation provisions, respectively. In April 2010, Dr. Isa Odidi offered and agreed to amend his employment agreement effective as of December 1, 2009, to eliminate the right to annual increases in his base salary of twenty per cent each year; and agreed to roll back his base salary effective December 1, 2009 to the level payable under the employment agreement for the period from September 2008 to August 2009, being C$452,000 per year.  Under this amendment, the base salary is open to potential increase on an annual basis at the discretion of the Board and Dr. Isa Odidi is eligible to receive a performance bonus, based on the performance, including that of Dr. Odidi and the Company, as may be determined in the discretion of the Board.

 

 

 

 

 

	Option-based Awards				Share-based Awards
Name	Number of securities underlying unexercised options (#)	Option exercise price	Option expiration date	Value of unexercised in-the-money options	Number of shares or units of shares that have not vested (#)	Market or payout value of share- based awards that have not vested
(a)	(b)	(c)	(d)	(e)(2)	(f)	(f)
Drs. Isa Odidi and Amina Odidi(1)	2,763,940	3.62	Sept. 10, 2014	N/A	N/A	N/A
Shameze Rampertab	60,000	C$2.62	Nov. 29, 2020	Nil	N/A	N/A
Graham Neil	25,000	C$3.62	Mar. 26, 2011	Nil	N/A	N/A

 

Notes

 

(1)	These option-based awards are held jointly.

 

(2)	The value of unexercised options at year end is calculated by subtracting the option exercise price from the closing price of the common shares of the Company on the TSX on November 30, 2010 (C$2.58) and multiplying the result by the number of common shares underlying an option.

 

 

Name	Option-based awards - Value vested during the year (U.S.$)	Share-based awards - Value vested during the year (U.S.$)	Non-equity incentive plan compensation - Value earned during the year (U.S.$)
(a)	(b)(1)	(c)	(d)
Dr. Isa Odidi	Nil	N/A	Nil
Dr. Amina Odidi	Nil	N/A	Nil
Shameze Rampertab	Nil	N/A	Nil
Graham Neil	Nil	N/A	Nil

 

 

(1)	The amount represents the theoretical total value if the options had been exercised on the vesting date, established by calculating the difference between the closing price of the common shares of the Company on the TSX and the exercise price.

 

 

 

 

 

 

 

Name	Fees earned	Share- based awards(1)	Option- based awards(2)	Non-equity incentive plan compensation	Pension value	All other compensation	Total
(a)	(b)	(c)	(d)	(e)	(f)	(g)	(h)
Eldon Smith	C$13,000	C$13,000	C$18,168	N/A	N/A	N/A	C$44,168
Kenneth Keirstead	C$26,000	N/A	C$18,168	N/A	N/A	N/A	C$44,168
Bahadur Madhani	C$28,000	N/A	C$18,168	N/A	N/A	N/A	C$46,168

 

Notes:

 

(1)	Deferred Share Units were earned but not granted as at November 30, 2010.

(2)

Option-based awards are options that were earned but not granted as at November 30, 2010. The value of option-based awards was estimated at November 30, 2010 using the Black-Scholes Option Pricing Model based on the closing price on the TSX at November 30, 2010 (C$2.58) with the following assumptions: volatility 98%, risk-free interest rate 2.25%, expected life 8.3 years, and no dividend yield.